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Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff

BACKGROUND/AIMS: New classes of cancer drugs bring a range of unknown and undesirable adverse events. Adverse event monitoring is essential in phase I trials to assess toxicity and safety. In phase II, the focus is also on efficacy but robust data on adverse events continue to inform the safety and...

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Autores principales: Kennedy, Fiona, Shearsmith, Leanne, Ayres, Michael, Lindner, Oana C, Marston, Lewis, Pass, Alison, Danson, Sarah, Velikova, Galina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE Publications 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8010887/
https://www.ncbi.nlm.nih.gov/pubmed/33231103
http://dx.doi.org/10.1177/1740774520972125
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author Kennedy, Fiona
Shearsmith, Leanne
Ayres, Michael
Lindner, Oana C
Marston, Lewis
Pass, Alison
Danson, Sarah
Velikova, Galina
author_facet Kennedy, Fiona
Shearsmith, Leanne
Ayres, Michael
Lindner, Oana C
Marston, Lewis
Pass, Alison
Danson, Sarah
Velikova, Galina
author_sort Kennedy, Fiona
collection PubMed
description BACKGROUND/AIMS: New classes of cancer drugs bring a range of unknown and undesirable adverse events. Adverse event monitoring is essential in phase I trials to assess toxicity and safety. In phase II, the focus is also on efficacy but robust data on adverse events continue to inform the safety and the adverse event profile. Standard, clinician-led monitoring has been shown to underestimate patients’ symptoms. Hence, patient-reported adverse event monitoring has been argued to complement and improve the information on adverse events in early phase clinical trials. With advances in information technology, real-time patient self-reported adverse events in trials are feasible. This study explored the experiences and procedures for reporting adverse events in early phase trials among patients, clinical staff, and trial staff, and their views on using an electronic patient-reported outcome adverse event system in this setting. METHODS: Qualitative interviews were conducted with patients, purposively sampled across ages, gender, and different phases of trials, and with clinical and trial-related staff involved in early phase trials (e.g. consultants, research nurses, hospital-based trial assistants/data managers, trial unit management staff). Interviews explored patient experiences and views on current adverse event reporting processes and electronic patient-reported outcome adverse event reporting. Framework analysis techniques were used to analyse the data. RESULTS: Interviewees were from two hospital trusts with early phase portfolios in England and a trial unit, and included sixteen patients, five consultants, four research nurses, five hospital-based trial staff, and two trial unit staff. Interviews identified three key themes (patient experiences, data flow, and views on electronic patient-reported outcome adverse event reporting). Stakeholders emphasised the intensity of trials for patients and the importance of extensive information provision within the uncertainty of early phase trial drugs. Regular face-to-face appointments for patients supplemented by telephone contact aimed to capture any adverse events. Delayed or under-reporting of mild- or low-severity symptoms was evident among patients. Hospital-based staff highlighted the challenges of current data collection including intense timescales, monitoring by trial sponsors, and high workload. Positive views on electronic patient-reported outcome adverse events highlighted that this could provide a more comprehensive and accurate view on the side effects of new drugs. Clinical staff emphasised patient safety and the need for clear responsibilities for monitoring. The need for careful decision-making about data flow and symptom attribution was highlighted; with trial unit staff emphasising the need for clinician review. CONCLUSION: Technology advances mean it is timely to explore the benefits and challenges of electronic patient-reported outcome adverse event reporting. This is a complex area warranting further consideration within the trial community. We have developed an online patient self-reporting tool and a small pilot with early phase trial patients is underway.
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spelling pubmed-80108872021-04-08 Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff Kennedy, Fiona Shearsmith, Leanne Ayres, Michael Lindner, Oana C Marston, Lewis Pass, Alison Danson, Sarah Velikova, Galina Clin Trials Articles BACKGROUND/AIMS: New classes of cancer drugs bring a range of unknown and undesirable adverse events. Adverse event monitoring is essential in phase I trials to assess toxicity and safety. In phase II, the focus is also on efficacy but robust data on adverse events continue to inform the safety and the adverse event profile. Standard, clinician-led monitoring has been shown to underestimate patients’ symptoms. Hence, patient-reported adverse event monitoring has been argued to complement and improve the information on adverse events in early phase clinical trials. With advances in information technology, real-time patient self-reported adverse events in trials are feasible. This study explored the experiences and procedures for reporting adverse events in early phase trials among patients, clinical staff, and trial staff, and their views on using an electronic patient-reported outcome adverse event system in this setting. METHODS: Qualitative interviews were conducted with patients, purposively sampled across ages, gender, and different phases of trials, and with clinical and trial-related staff involved in early phase trials (e.g. consultants, research nurses, hospital-based trial assistants/data managers, trial unit management staff). Interviews explored patient experiences and views on current adverse event reporting processes and electronic patient-reported outcome adverse event reporting. Framework analysis techniques were used to analyse the data. RESULTS: Interviewees were from two hospital trusts with early phase portfolios in England and a trial unit, and included sixteen patients, five consultants, four research nurses, five hospital-based trial staff, and two trial unit staff. Interviews identified three key themes (patient experiences, data flow, and views on electronic patient-reported outcome adverse event reporting). Stakeholders emphasised the intensity of trials for patients and the importance of extensive information provision within the uncertainty of early phase trial drugs. Regular face-to-face appointments for patients supplemented by telephone contact aimed to capture any adverse events. Delayed or under-reporting of mild- or low-severity symptoms was evident among patients. Hospital-based staff highlighted the challenges of current data collection including intense timescales, monitoring by trial sponsors, and high workload. Positive views on electronic patient-reported outcome adverse events highlighted that this could provide a more comprehensive and accurate view on the side effects of new drugs. Clinical staff emphasised patient safety and the need for clear responsibilities for monitoring. The need for careful decision-making about data flow and symptom attribution was highlighted; with trial unit staff emphasising the need for clinician review. CONCLUSION: Technology advances mean it is timely to explore the benefits and challenges of electronic patient-reported outcome adverse event reporting. This is a complex area warranting further consideration within the trial community. We have developed an online patient self-reporting tool and a small pilot with early phase trial patients is underway. SAGE Publications 2020-11-24 2021-04 /pmc/articles/PMC8010887/ /pubmed/33231103 http://dx.doi.org/10.1177/1740774520972125 Text en © The Author(s) 2020 https://creativecommons.org/licenses/by/4.0/ This article is distributed under the terms of the Creative Commons Attribution 4.0 License (https://creativecommons.org/licenses/by/4.0/) which permits any use, reproduction and distribution of the work without further permission provided the original work is attributed as specified on the SAGE and Open Access page (https://us.sagepub.com/en-us/nam/open-access-at-sage).
spellingShingle Articles
Kennedy, Fiona
Shearsmith, Leanne
Ayres, Michael
Lindner, Oana C
Marston, Lewis
Pass, Alison
Danson, Sarah
Velikova, Galina
Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff
title Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff
title_full Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff
title_fullStr Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff
title_full_unstemmed Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff
title_short Online monitoring of patient self-reported adverse events in early phase clinical trials: Views from patients, clinicians, and trial staff
title_sort online monitoring of patient self-reported adverse events in early phase clinical trials: views from patients, clinicians, and trial staff
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8010887/
https://www.ncbi.nlm.nih.gov/pubmed/33231103
http://dx.doi.org/10.1177/1740774520972125
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